Fetuin-A Induces Cytokine Expression and Suppresses Adiponectin Production

A Kappes; A Santoliquido; A Siddiq; AH Kissebah; Alessandro Bartolomucci; Andreas Fritsche; Anita M. Hennige; AS Lihn; B Denecke; B Iglseder; C Lara-Castro; C Schafer; C Weyer; Corinna Wicke; D Rothenbacher; DC Chan; DR Matthews; EE Kershaw; F Bacha; Fausto Machicao; FF Fisher; G Rauth; H Xu; Hans-Ulrich Häring; Harald Staiger; I Dahlman; JH Ix; JM Bruun; JM Lyles; K Hara; K Mori; K Mori; KM Dziegielewska; KO Pedersen; KS Lam; M Fasshauer; M Fasshauer; M Ketteler; M Roden; MB Schulze; ME Trujillo; N Stefan; N Stefan; N Vionnet; Norbert Stefan; O Tschritter; P Auberger; P Ruminy; P Schling; PR Srinivas; SP Weisberg; ST Mathews; ST Mathews; ST Mathews; T Kadowaki; T Pischon; TI Pollin; TS Tsao; VR Sopasakis; W Jahnen-Dechent; W Schmidt; X Lin

Fetuin-A Induces Cytokine Expression and Suppresses Adiponectin Production

Abstract

BACKGROUND: The secreted liver protein fetuin-A (AHSG) is up-regulated in hepatic steatosis and the metabolic syndrome. These states are strongly associated with low-grade inflammation and hypoadiponectinemia. We, therefore, hypothesized that fetuin-A may play a role in the regulation of cytokine expression, the modulation of adipose tissue expression and plasma concentration of the insulin-sensitizing and atheroprotective adipokine adiponectin. METHODOLOGY AND PRINCIPAL FINDINGS: Human monocytic THP1 cells and human in vitro differenttiated adipocytes as well as C57BL/6 mice were treated with fetuin-A. mRNA expression of the genes encoding inflammatory cytokines and the adipokine adiponectin (ADIPOQ) was assessed by real-time RT-PCR. In 122 subjects, plasma levels of fetuin-A, adiponectin and, in a subgroup, the multimeric forms of adiponectin were determined. Fetuin-A treatment induced TNF and IL1B mRNA expression in THP1 cells (p<0.05). Treatment of mice with fetuin-A, analogously, resulted in a marked increase in adipose tissue Tnf mRNA as well as Il6 expression (27- and 174-fold, respectively). These effects were accompanied by a decrease in adipose tissue Adipoq mRNA expression and lower circulating adiponectin levels (p<0.05, both). Furthermore, fetuin-A repressed ADIPOQ mRNA expression of human in vitro differentiated adipocytes (p<0.02) and induced inflammatory cytokine expression. In humans in plasma, fetuin-A correlated positively with high-sensitivity C-reactive protein, a marker of subclinical inflammation (r = 0.26, p = 0.01), and negatively with total- (r = -0.28, p = 0.02) and, particularly, high molecular weight adiponectin (r = -0.36, p = 0.01). CONCLUSIONS AND SIGNIFICANCE: We provide novel evidence that the secreted liver protein fetuin-A induces low-grade inflammation and represses adiponectin production in animals and in humans. These data suggest an important role of fatty liver in the pathophysiology of insulin resistance and atherosclerosis

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